D-homosteroids and process for their preparation



United States Patent US. Cl. 260488 25 Claims ABSTRACT OF THE DISCLOSURE A compound of the formula wherein each of R and R is hydrogen and R and R together represent a methylene group, X is a member selected from the group consisting of hydrogen, lower alkyl, chlorine and fluorine, and AB is selected from the group of R 0 l on,

and

h) H C\ OR; 17:: 0;,

in which R and R are each selected from the group 40 consisting of hydrogen and acyl, and the process of preparing such compound Which comprises contacting a compound of the formula esterified hydroxyl group is saponified and, if desired, this saponified group is reesterified.

The invention is directed to D-homosteroids constitut- 5 ing androgen antagonists having the formula wherein R and R are hydrogen or, taken together, form a methylene group, X is hydrogen, lower alkyl, fluorine or chlorine, and AB preferably represents the group R 0 CH; 0

wherein R and R are hydrogen or acyl. The D-homosteroids of the above formula are prepared by treating compounds of the formula i=0 ,HN OH I O X II wherein R R and X are as defined above with a basic or acid catalyst, and depending on the meaning of R and R in the final product as defined above, if desired, in the resulting compound any free hydroxyl group is esterified or any esterified hydroxyl group is saponified and, if desired, this saponified group is reesterified.

The present invention relates to novel D-homosteriods having androgen antagonistic properties, compositions including the same as active ingredient, and a process for preparing the novel compounds.

A large number of homosteroid compounds having a broad range including very different properties have been described. D-homosteroids characterized by specific androgen antagonistic activity, however, are not as yet known.

It is therefore an object of the present invention to provide D-homosteroids characterized by androgen antagonist activity.

It is a further object of the present invention to provide a process for the preparation of D-homosteroids having androgen antagonist activity.

It is another object of the present invention to provide a method for use in the treatment of diseases and disorders caused by or connected with androgens.

It is still another object of the present invention to provide compositions containing an effective amount of a D-homosteroid having androgen antagonist activity.

Other objects will become apparent from the following description:

In accordance with the invention it has been found that D-homosteroids of the formula wherein R and R are hydrogen or acyl, have utility as androgen antagonists.

The D-homosteroids as set out above are characterized by particularly marked androgen antagonistic activity and are therefore of value as therapeutic agents in those instances where a high degree of androgen antagonistic activity is desired. The properties of the D-homosteroids according to the present invention can be modified by the conventional procedures as, for instance, by introduction of different groups into the molecule of the compound designated by Formula I above. Thus, in addition to hydrogen, fluorine or chlorine, X may be a lower alkyl group having from 1 to 8 carbon atoms and preferably from 1 to carbon atoms. R and R, can be hydrogen or an acyl group and, in the latter case, designate esterified residues of the common inorganic acids, such as sulfuric acid, phosphoric acid, and the like; or designate the group RCO wherein R is a branched or unbranched alkyl or alkenyl group or an aromatic or hydroaromatic group, in which connection all of said groups may be monoor poly-substituted, the substituent preferably being a halo, hydroxy, carboxy, or amino group. Consequently the acyl groups having preferably 1 to 12 carbon atoms may be esterified residues of the following aliphatic, monoor dicarboxylic acids, such .as acetic acid, propionic acid, isobutyric acid, caproic acid, caprylic acid, yalerianic acid, onanthic aid, undecanoic acid, undecylenic acid, malonic acid, fumaric acid, glutaric acid, and the like. The aforementioned aliphatic acids may be substituted, preferably by halogen, as for instance chlorine, or by hydroxy, or amino groups. Instances of aliphatic acids of this type include mono and dichloroacetic acid, glyceric acid, hydroxy and amino propionic acid, and the like.

The substituted or unsubstituted aromatic acyl groups of the following acids are included within the scope of the invention: benzoic acid, nicotinic acid, and the like.

In accordance with the invention, the new D-homosteroids can be prepared from starting materials having the Formula H wherein R R and X are as defined above by treating such starting materials with catalysts, i.e., acid or basic catalysts, whereby the configurations are obtained and depending on the meaning of R and R in the final product as defined above, if desired, in the resulting compound any free hydroxyl group is esterified or any esterified hydroxyl group is saponified and, if desired, this saponified group is reesterified.

The starting materials of Formula II can be obtained by the method described in US. Patent 3,234,093; German Patent 1,189,991; US. Patent 3,127,396; US. Patent 3,138,589, and US. Patent 3,042,688.

As has been set out above, the conversion of the l7-hydroxy-20-ketones to the corresponding D-homosteroids is effected by treatment with a basic or acid catalyst. Depending on the basic or acidic character of the catalyst used, D-homosteroids are obtained which differ one from the other with respect to the position of the keto group and the position and the stearic configuration of the hydroxyl group.

The enlargement of the D-ring to the D-homosteroid- 17-ketone is preferably effected using basic catalysts, such as alkaline earth hydroxides, for instance, magnesium hydroxide, calcium hydroxide, strontium hydroxide, barium hydroxide or basic aluminum oxide. When the reaction is catalyzed by basic aluminum oxide, the same is advantageously conducted in such a manner that the basic aluminum oxide and the steroid used as starting material are maintained in contact with one another for a longer period of time, the contacting being effected in the presence of a non-polar solvent such as benzene. Following completion of this phase of the reaction, the D-hornosteroid formed is extracted from the reaction mixture using polar solvent such as methanol, ethanol, acetone, acetic acid ester, chloroform, or the like.

The reaction when etfected with alkaline earth hydroxides takes place most advantageously in alcoholic suspension, preferably in methanol, at the boiling temperature of the alcohol used. Alkali-metal hydroxide, such as lithium hydroxide, is, in principle, suitable for use as basic catalysts, but their use is less advantageous in those cases where halogen compounds are involved.

The acid catalyst transposition to the l'l-wketones takes place, for example, in the presence of Lewis acids, such as boron trifluoride etherate or aluminum alkoxides as, for example, aluminum tert.butylate. When aluminum alkoxides are employed, the reaction mixture is heated, preferably in the presence of a solvent such as benzene, toluene or xylene, the 17-tx-hydroxy compound being thereby obtained in excellent yield.

The reaction, when catalyzed by boron trifluoride, proceeds most advantageously in the presence of acetic acid as solvent and in the presence of acetic acid anhydride. Under the aforesaid conditions, the 17-wacetoxy compound is obtained, the boron trifluoride is preferably used in the form of its etherate, although other solvents than ethers, such as benzene, toluene, tetrahydrofuran or dioxan may be used.

As has been noted above, the D-homosteroids according to the present invention and, in particular, the l7-ketones obtained by alkaline conversion constitute highly active androgen antagonistic agents. The androgen antagonistic activity of the compounds of the invention was evaluated in a test procedure employing one-day old male chicks, i.e., cockscomb. The animals were maintained for a period of 7 days on 0.1 mg. testosterone propionate per day and simultaneously were given graduated doses of the test compound either intramuscular or perorally. On the eighth day, the animals were killed and the weight of both the animal and of the comb was separately determined. The degree of the androgen antagonist effect is measured by the quotient of the comb Weight in milligrams2body weight in grams, the values which were determined being set out in the following Tables I and II. The untreated controls as can be seen from the tables have a small quotient (0.33) whereas animals who had been treated only with testosterone propionate have a high quotient (1.13). The smaller the quotient obtained in those animals which received both testosterone propionate and an androgen antagonist, the stronger is the androgen antagonist activity of the compound employed. In the following tables the effect of the D-homosteroid (IV) according to the present invention as compared with the activity of two compounds (I) and (II) comprises known androgen antagonists and of the starting material (III) which itself constitutes an androgen antagonist, can be seen.

TAB LE 1 Dosage in mg, Quotient, Combanimal/day of weight, mg./

Substance 7 x i.m. test substance Body weight, g.

Untreated controls 0 0 33 0.1 mg. Testosteronepropionate (I)A -testoIactone 10. 0 0.92 +0.1 mg. 'IP 3. 0 1.00

(II) Progesterone. 10.0 0. 48 +0.1 mg. 'IP 3.0 0.77

(III) ochloro-lfla-methylene 3. 0 0.76 A -pregnadienel7a-o1 1. 0 0. 87 3,20-dione 0.3 0 98 +0.1 mg. TP.

(IV) fi-chloro-liaa-methyl-l,Zu 1.0 0.30 methyleneD-homo-A --andro 0. 3 0. 51 stadiene-l7afl-o1-3,17 dione +0.1 0. 1 0. 79 mg. TI.

TAB LE II Dosage in mg, Quotient, Combanimal/day of weight mg./

Substance 7 x p.0. test substance Body weight, g.

(IDProgesterone 10 0 0.98 +0.1 mg TP 3. 0 I. 29

(III) 6-chloro-1,2a-methylene- 10.0 0.78 A -preguadiene-Haol-3,20-dione 3. 0 1. 62 +0.1 mg.IP.

(IV) G-chloro-lTawmethyLl,Za- 3. 0 0.38 methyleue-D-homo A -andro- 1.0 0.51 stadiene-17aBpl-3,17-dione +0.1 0.3 0. 61 mg. TP. 0. 1 0. 73

D-homosteroids having androgen antagonistic activity have heretofore not been described. The above tables illustrate that the transposition of the C side chain (III) to the D-homosteroid (IV) causes an increase in activity amounting to between 30 to 100.

Because of the testosterone antagonism manifested by the steroids according to the invention, these compounds can be used in the treatment of all diseases and conditions which are caused by, or associated with, an androgen hyper-production, such as infantile acne vulgaris, and hirsutism. The compounds of the invention can be administered both subcutaneously, intramuscularly, or orally.

The preparation of the actual therapeutic agents is carried out by the methods of the art. The active agents are formulated together with the usual ingredients, such as carriers, taste improvement agents, dispersants, and the like. For parenteral application, oily solutions prepared using sesame or castor-oil are preferred. In addition to the oil, agents increasing the solubility, i.e., solubilizing or dissolution aids, may be incorporated as, for example, benzyl benzoate or benzyl alcohol. For oral administration, the compounds can be used in the form of tablets, drages, capsules, pills or as liquids, i.e., suspensions or solutions.

Tablets constitute a preferred mode of administration. A typical formulation is set out hereinafter 6 Active substance:

6 chloro 17aa methyl 1,2a methylene- D homo A -androstadiene 17afi ol- 3,l7-dione mg 10.000 Filling agent:

Cornstarch (USP 16) mg 66.565 Lactose (DAB 6) mg 36.000 Talcum (DAB 6) mg 6.000 Gelatine, white (DAB 6) mg 1.400 Preservative:

p Hydroxy benzoic acid methylester (DAB 6, 3rd supplement) 24 p Hydroxy benzoic acid propylester (DAB 6, 3rd supplement) 11 Weight of tablet mg 120.000

The tablets are prepared in the conventional manner from the above formulation using the conventional equipment.

The dosage of the compounds as set out herein depends on the condition which is being treated as well as the effect sought to be realized. Generally, 20 to 200 mg. of active substance are given in 3 to 15 divided doses per day in treating diseases caused by androgen production or which are connected with such androgen production.

In clinical treatment it has been observed that after 3 months an improvement or alleviation of the condition has taken place.

In order that the invention may be more fully understood, reference should be had to the following specific examples in which are disclosed the compounds and processes coming within the scope of the present invention. It will be understood that these examples are given for illustrative purposes merely and are not intended as limitations of the invention:

EXAMPLE 1 5.0 g. 6-chloro-1,Zia-methylene-A -pregnadiene-l7u-ol- 3,20-dione in benzene were adsorbed on a fifty-fold amount of basic aluminum oxide containing 1% of Water. After a reaction time of 24 hr. the reaction product was extracted with methanol, which was then evaporated to dryness in vacuo. The residue was recrystallized from methanol with the addition of methylene chloride. The yield of 6-chloro-1Jot-methylene-17aa-methyl-D-homo- M -androstadiene-l7afi-ol-3,17-dione having a melting point of 265-268 C. (decomposition) amounted to 1.2 g.

300 mg. 6-chl0ro-1,2tx-methylene-17aa-methyl-D-homon -androstadiene-17a,B-ol-3,17-dione were stirred for 17 hours at room temperature in 6 ml. glacial acetic acid with 3 ml. acetic acid anhydride and mg. p-toluenesulfonic acid. Afterwards the reaction mixture was poured into ice-water/pyridine with stirring, the precipitate separated by suction, washed till neutral and dried. After recrystallization from methanol 210 mg. 6-chloro-l,2amethylene 17am methyl D homo A androstadiene-l7a5-ol-3,17-dione-17a-acetate were obtained having a melting point of 272274 C.

400 mg. 6-Ch1010-1,ZOL-HlfithYlGl'lC-l7aOt-II1Cthy1-D-hOIIlO- A -androstadiene-l7afi-ol-3,l7-dione were stirred in 8 ml. propionic acid with 4 ml. propionic acid anhydride and 200 mg. p-toluene-sulfonic acid for 10 hours at room temperature. The reaction mixture was stirred in ice water/pyridine, the precipitate separated by suction, dissolved in methylene-chloride, washed with sodium-bicar bonate-solution and water, and dried over sodium sulfate. After evaporation to dryness, the residue was recrystallized from isopropyl ether. The yield amounted to 320 mg. 6 chloro 1,20: methylene 17am methyl D- homo A androstadiene 17afi ol 3,17 dione 17apropionate having a melting point of 212213.5 C.

7 EXAMPLE 2 3,0 g. 6-fluoro-1,Za-methylene-A -pregnadiene-17a-o1- 3,20-dione were adsorbed on basic aluminum oxide and then worked up as described in Example 1.

6 fiuoro 1,2 methylene 1721a methyl D homo- A -androstadiene-17a,8-ol-3,17-dione were recovered.

UV: E38D=19.000.

350 mg. 6-fil10l0-1,ZOt-HlfithYlCIlC-17fl0t-H1GthYl-D-h0l110- A -androstadiene-17a/3-ol-3,l7-dione were stirred in 7 ml. glacial acetic acid and 3.5 ml. acetic acid anhydride and 175 mg. p-toluenesulfonic acid added thereto, and the mixture worked up as described in Example 1.

6 fluoro 1,20: methylene 17am methyl D homo- A -androstadiene-l7afi-ol-3,l7-dione-17a-acetate were recovered.

400 mg. 6-fluoro-l,2a-methylene-17aa-methyl-D-homo- A -androstadiene-Nasal-3,l7-dione were stirred in 4 ml. caproic acidanhydride with 200 mg. p-toluenesulfonic acid for 24 hours at room temperature. After icewater precipitation, the precipitate was stirred by suction and dissolved in methylene chloride, the methylene-chloride solution was washed with sodium bicarbonate solution and water and then evaporated to dryness in vacuo after drying over sodium sulfate. There were recovered 6-fillOIO-1,ZOt-ITIBlLhYlBDG-173a-methyl-D-h0l'I1OA -Z1Ild1'O stadiene-l7a/3-ol-3,l7-dione-l7a-capronate in the form of an oil.

UV: e 18.600.

EXAMPLE 3 2.5 g. 6-chloro-M -pregnadiene-17a-ol-3,20-dione were adsorbed in basic aluminum oxide and worked up according to Example 1.

There were recovered 6-chloro-l7aa-methyl-D-homo- A -androstadiene-l7ai3-ol-3,17-dione.

400 mg. 6-chloro-l7am-methyl-M' -D-homo-androstadiene-17afl-ol-3,17-dione were reacted and worked up according to Example 1 in 8 ml. glacial acetic acid with 4 m1. acetic acid anhydride and 200 mg. p-toluenesulfonic acid.

There were recovered 6-chloro-l7aa-methyl-D-hornod -androsta'diene-17afl-ol3,17-dione17a-acetate.

EXAMPLE 4 4.0 g. 1,Za-methyIene-A -pregnadiene-17a-ol'3,20-dione were adsorbed on basic aluminum oxide and worked up according to Example 1.

There were recovered 850 mg. 1,2a-methylene-17aamethyl D homo A androstadiene 173.5 ol 3,17- dione having a melting point of 2635-268 C.

300 mg. 1Jot-methylene-l7aa-methyl-D-homo-A -androstadiene-17aB-ol-3,17-dione were reacted and worked up according to Example 1 in 6 ml. glacial acetic acid with 3 ml. acetic acid anhydride and 150 mg. p-toluenesulfonic acid according to Example 1.

There were recovered 1,Za-methylene-l7aot-methyl-D- hom-A -androstadiene-17a,8-ol-3,17-dione-17a-acetate.

EXAMPLE 4.0 g. fi-methyl-d -pregnadiene-17a-ol-3,20-dione were adsorbed on basic aluminum oxide and worked up according to Example 1.

There were recovered 6,l7aor-dirnethyl-D-homo-A androstadiene-17afi-ol-3,17-dione.

UV: 2gu=24.000.

500 mg. 6,17aa-dimethyl-Dhomo-A -androstadiene- 17afl-ol-3,17-dione were reacted and worked up according to Example 1 in ml. glacial acetic acid with 5 ml. acetic acid anhydride and 250 mg. p-toluene-sulfonic acid.

There were recovered 6,17aa-dimethyl-D-homo-A androstadienel7afi-ol- 3 ,17-dione-17a-acetate.

UV: 290=24.1O0.

EXAMPLE 6 1.0 g. 6-chloro-1,2m-methylene-A -pregnadiene-17aol-3,2 0-dione were refluxed with stirring in 150 ml. methanol with 10.0 g. barium-hydroxide for 3 hours. Thereafter the solids were rinsed by filtration, the solution concentrated in vacuo, taken up in methylene-chloride and washed with water. After drying over sodiumsulfate and evaporating to dryness, the residue was recrystallized from methanol with the addition of methylenechloride. There were recovered 210 mg. 6-chloro-l,2u-methylene- 1721a methyl D homo A androstadiene 17a;8 ol-3,17-dione having a melting point of 264-267 C.

EXAMPLE 7 300 mg. 6-fluoro-LZm-methylene-A -pregnadiene-17aol-3,20-dione were reacted and worked up in ml. methanol with 8.0 g. bariumhydroxide as described in Example 6. There were recovered 6-fluoro-l,2a-methylene-17aa-methyl-D-homo-d -androstadiene-l7a fi-ol-3, 17- dione.

UV: e =18.300.

EXAMPLE 8 1.1 g. 6-chloro-A -pregnadiene-17a-ol-3,20-dione Were reacted and worked up in ml. methanol with 11. 0 g. strontium-hydroxide according to Example 6.

There were recovered 6-chloro-17aa-methyl-D-homod -androstadiene-17afi-ol-3,17-dione.

UV: 6281:2L3O0.

EXAMPLE 9 500 mg. 1,Za-methyIene-A -pregnadiene-l7a-ol-3,20 dione were reacted and worked up in 70 ml. methanol with 5.0 g. bariumhydroxide according to Example 6.

There were recovered 110 mg. 1,2a-methylene-l7aamethyl D homo A androstadiene 17afi ol 3,17 dione having a melting point of 265-268 C.

EXAMPLE 10 600 mg. 6 methyl A pregnadiene 17a o1 3,20 dione were reacted and worked up in 90 ml. methanol with 6.0 g. strontiumhydroxide according to Example 6.

6,17aa dimethyl D homo A androstadiene 1721 3 ol 3,17 dione were recovered.

UV: 240=16.1OO.

EXAMPLE 1 1 2 g. 6 chloro 1,2 methylene A pregnadiene 17a ol 3,20 dione were refluxed in 400 ml. toluene with 2 g. aluminum tert.-butylate for 2 hours. The reaction mixture was cooled and thereafter treated with ice and as much 5% hydrochloric acid as necessary to dissolve the precipitated aluminum-hydroxide. The organic phase was separated, washed with water, dried over sodiumsulfate and evaporated. The residue was chromatographed on aluminum oxide and recrystallized from methanol.

0.75 g. 6 chloro 1,2m methylene 17,3 methyl D homo A androstadiene 17a ol 3,17a dione having a melting point of 230-231 C. was recovered.

EXAMPLE 12 200 mg. 6 chloro 1,20: methylene A pregnadiene 17oz. ol 3,20 dione were kept for 24 hours at room temperature in 40 ml. benzene absolute and 0.4 ml. borontrifluoride etherate. The reaction mixture was decomposed with ice-water, the organic phase extracted with methylene chloride and the extract washed, dried and evaporated. After recrystallization from methanol, mg. 6-chloro-l,Za-methylene-17fi-methyl-D-homo-a -androstadiene-17a-ol-3,l7adione having a melting point of 230-231 C. were obtained.

EXAMPLE 13 4.0 g. 6 chloro 1,241 methylene A pregnadiene 17oz ol 3,20 dione were kept in 200 ml. glacial acetic acid with 4 .ml. acetic acid anhydride and 4 ml. borontrifluoride-etherate for 3 days at room temperature. Thereafter the mixture was stirred into ice-water, the precipitate removed by suction, washed with water and taken up with methylene-chloride. After drying over sodiumsulfate and evaporating to dryness and recrystallizing from methanol, 3.9 g. 6cl1loro-1,2a-methylene-17B- methyl D homo A androstadiene 17a ol 3,170: dione 17 acetate having a melting point of 262.5263 C. were obtained 1.8 g. 6 chloro 1,20; methylene 17B methyl D homo A androstadiene 17oz ol 3,17m dione 17 acetate were stirred in 350 ml. methanol with 28.8 ml. sodium hydroxide solution for 24 hours at room temperature. After neutralization with acetic acid the solution was substantially evaporated in vacuo. Thereafter it was diluted with water, the precipitate separated by suction, washed with water and taken up in methylene-chloride. After drying over sodium sulfate, evaporating to dryness and recrystallizing from methanol, 1.2 g. 6-Chl0I'O-1,2amethylene 17,8 methyl D homo A androstadiene 17a ol 3,17a dione having a melting point of 230-231 C. were obtained.

UV: e =17.500.

400 mg. 6 chloro 1,20; methylene 17,8 methyl D homo A androstadiene 17cc ol 3,170; dione were kept in 8 ml. propionic acid with 4 ml. propionic acid anhydride and 200 mg. p-toluenesulfonic acid for 24 hours at room temperature. After ice-water precipitation, the precipitate was separated off, taken up with methylenechloride, washed with sodium bicarbonate solution and water and dried over sodium sulfate. Thereafter the solution was evaporated to dryness in vacuo and the residue recrystallized from isopropyl ether.

310 mg. 6 chloro 1,2 methylene 17B methyl D homo A androstadiene 17a ol 3,17a dione 17 propionate having a melting point of 165-165.5 were recovered.

UV: 62g =17.l00.

EXAMPLE 15 3.0 g. 6 fiuoro 1,2a methylene A pregnadiene- 17cc ol 3,20 dione were reacted and worked up in 150 ml. glacial acetic acid with 3 ml. acetic acid anhydride and 3 ml. borontrifluoride etherate according to Example 14.

After recrystallization from methanol there were recovered 2,9 g. 6-fiuoro-1,2a-methylene-17/3-methyl-D-homo- A -androstadiene-17ot-ol-3,17a-dione-17-acetate having a melting point of 219.5-220.5 C.

1.5 g. 6-f1uoro-1,2a-methylene-17/3-methyl-D-homo-A androstadiene-1711-01-3,l7a-dione-17-acetate were reacted in 200 ml. methanol with 24 ml. 1 N sodium hydroxide solution according to Example 14.

After recrystallization from acetic acid ester amounted to 1.2 g. 6-fiuoro-1,2a-methylene-17fi-methyl-D-homo- A -androstadiene-17ix-ol-3,17a-dione having a melting point of 205-206 C.

500 mg. 6-fluoro-l,2a-methylene-17;3-methyl-D-homod -androstadiene-17u-ol-3,l7a-dione were stirred into 5 ml. caproic acidanhydride with 250 mg. p-toluenesulfonic acid for 4 days at 37 C. After steam-distillation, the aqueous phase was extracted with methylene chloride and dried over sodium sulfate. After evaporation to dryness and chromatographing on silica-gel, 450 mg. 6-fluor0-1,2a methylene-17B-methyl-D-homo-A androstadiene 17ao1-3,17a-dione-17-capronate in the form of an oil were obtained.

UVIE280=18.500.

EXAMPLE 16 4.0 g. 6-chloro-A -pregnadiene-17u-ol-3,20-dione were reacted and worked up in 200 ml. glacial acetic acid with 4 ml. acetic acid anhydride and 4 ml. borontrifluoride etherate according to Example 14.

After recrystallization from isopropyl ether, 3.1 6- chloro-17fl-methyl-D-homo-A -androstradiene-1711-01 3, l7a-dione-l7-acetate having a melting point of -1615 C. were obtained.

1.7 g. 6-chloro-17fi-methyl-D-homo-A -androstadiene- 17tx-ol-4,l7a-dione-17-acetate were reacted and worked up in 300 ml. methanol with 29 ml. 1 N sodium hydroxide solution according to Example 14. A yield of 1.2 g. 6- chloro-l7B-methyl-D-homo-A -androstadiene-17a-ol 3, 17a-dione having a melting point of 226.5227 C. was obtained.

EXAMPLE 17 3.5 g. 1,Zix-methylene-A -pregnadiene-17ot-ol 3,20- dione were reacted and worked up in glacial acetic acid with 3.5 ml. acetic acid anhydride and 3.5 ml. borontrifluoride etherate according to Example 14.

After recrystallization in methanol, 3.1 g. 1,2a-methy1- ene-17,8-methyl-D-homo-A -androstadiene-17a 01 3, 17a-dione-17-acetate having a melting point of 212.5- 213.5 C. were obtained.

UVIE231=21.500.

1.5 g. 1,2ot-methy1ene-17,8-methyl-D-homo-A androstadiene-17a-ol-3,17a-dione-17-acetate having a melting point of 200 ml. methanol with 24 ml. 1 N sodiumhydroxide solution according to Example 14 were obtained.

After recrystallization from acetic acid ester, 970 mg. 1,2ot-methylene-17,6-methyl-D-homo-A androstadienel7a-ol-3,l7a-dione having a melting point of 191192 C were obtained.

EXAMPLE 18 ll 11 0175 C and Q C 7 in which R and R are each selected from the group consisting of hydrogen and an aliphatic hydrocarbon carboxylic acid acyl having from 1 to 12 carbon atoms.

2. A compound according to claim 1 designated 6- chloro-l,2a-methylene 17aa-methyl-D-homo A androsta-dienel7a13-ol-3 l7-dione.

3. A compound according to claim 1 designated 6-chloro 1,20: methylene 17am methyl D= homo A androstadienel7a/3-ol-3 ,l7-dione-17a-acetate.

4. A compound according to claim 1 designated 6-ch1oro 1,2a methylene 17am methyl D homo A androstadiene- 1721;8-01-3, l7-dione-17a-propionate.

5. A compound according to claim 1 designated 6-fiuoro 1,20. methylene 173.0: methyl D homo A androstadiene-17a,B-ol-3,17-dione.

6. A compound according to claim 1 designated 6-fluor0 1,211 methylene 17am methyl D homo A androstadiene-l7aB-ol3,17-dione-l7a-aeetate.

7. A compound according to claim 1 designated 6-fluor0 1,2a methylene 17am methyl D homo A androstadiene-l7afi-ol-3,17-dione-17a-capronate.

8. A compound according to claim 1 designated 6-chloro 17aa methyl D homo A androstadiene l7aflol-3,l7-dione.

9. A compound according to claim 1 designated 6-chloro l7aa methyl D homo A androstadiene 17afl- 01-3, l7-dione-l7a-acetate.

10. A compound according to claim 1 designated 1,20:- methylene 17am methyl D homo A androstadiene-17afi-ol-3, l7-dione.

11. A compound according to claim 1 designated 1,20;- methylene 17am methyl D homo A androstadiene-l7a B-ol-3 ,17-dione-17a-acetate.

12. A compound according to claim 1 designated 6, 173.01. dimethyl D homo A androstadiene 17a,8- o1-3,17-dione.

13. A compound according to claim 1 designated 6, 17am dimethyl D homo A androstadiene 1721(3- 01-3,l7-dione-17a-acetate.

14. A compound according to claim 1 designated 6- chloro 1,211 methylene 17B methyl D homo A androstadiene-l7a-ol-3,17a-dione.

15. A compound according to claim 1 designated 6- 12 chloro 1,204 methylene methyl D homo A androstadienc- 1711-01-3, l7a-dionel 7-acetate.

16. A compound according to claim 1 designated 6- chloro 1,2a methylene 17 6 methyl D homo A androstadiene-17a-0l-3,17a-dione-l7-propionate.

17. A compound according to claim 1 designated 6-fiuoro 1,2m methylene 17B methyl D homo A androstadiene- 17a-0l-3 l 7a-dione-l7-acetate.

18. A compound according to claim 1 designated 6-fluoro 1,20; methylene 17B methyl D homo A- androstadiene-l7a-ol-3,17a-dione.

19. A compound according to claim 1 designated 6-fluoro 1,20: methylene 175 methyl D homo A- androstadiene-l7u-o1-3,l7a-dione-l7-capronate.

20. A compound according to claim 1 designated 6- chloro 17,9 methyl D homo A androstadienel7a-ol-3,l7a-dione-17-acetate.

21. A compound according to claim 1 designated 6- chloro 17,6 methyl D homo A androstadiene- 17a-0l-3,173.-dl0l'l6.

22. A compound according to claim 1 designated 1,2otmethylene 1719 methyl D homo A androstadiene-1701-01-3,l7a-dione-l7-acetate.

23. A compound according to claim 1 designated 1,20;- methylene 17B methyl D homo A androstadiene-l7a-ol-3,l7a-dione.

24. A compound according to claim 1 designated 6, 17,8 dimethyl D homo A androstadiene 17a ol- 3,17a-dione-l7-acetate.

25. A compound according to claim 1 designated 6, 17,8 dimethyl D homo A androstadiene 17oz o1- 3,17a-dione.

References Cited UNITED STATES PATENTS 9/1964 Moersch et a1 260-586 8/1966 Moersch et al 2605 86 OTHER REFERENCES Chem. Abstracts, 62:6535a (1965), Shoppee et a1. Helv. Chim. Acta., vol. 26 (1943), pp. 186-189, Wendler et al.

US. Cl. X.R. 

